肝细胞癌血管生成与侵袭性生物学相关，与肿瘤免疫原性相平衡。

IF 2.1 Q3 ONCOLOGY

World Journal of Oncology Pub Date : 2025-04-01 Epub Date: 2025-01-25 DOI:10.14740/wjon2009

Raj Vaghjiani, Rongrong Wu, Kaity H Tung, Takashi Ishikawa, Kazuaki Takabe

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引用次数: 0

摘要

背景：肝细胞癌（HCC）是一种动脉化肿瘤；因此，抗血管生成靶向治疗已进入临床实践阶段。在此，我们假设高血管生成的HCC具有生物侵袭性，生存率较差。方法：血管生成评分（AS）来源于分子特征数据库（MSigDB）贺曼血管生成基因集，用中位数划分高组和低组。分析Cancer Genome Atlas （TCGA, n = 386）和GSE76427 （n = 115）队列HCC患者的转录组。结果：AS高与血管生成相关基因表达相关。微血管和淋巴内皮细胞浸润在高血管生成的HCC中均较高。令人惊讶的是，不同水平的血管生成并没有发现生存差异。在基因集富集分析（GSEA）中，高血管生成显著富集了肿瘤加重信号通路：糖酵解、Notch、Hedgehog、KRAS、上皮间充质转化和转化生长因子-β (TGF-β)，但在两个队列中，CD8+ T细胞和T辅助1细胞的浸润量较少，M1巨噬细胞和常规树突状细胞（cDCs）的浸润量较高，细胞溶解活性评分升高。与此一致的是，免疫反应相关的基因集：炎症反应、肿瘤坏死因子α (TNF-α)信号、同种异体移植排斥反应、干扰素α和干扰素γ都在高血管新生HCC中富集。程序性细胞死亡蛋白1 （PD1）、程序性死亡配体1 （PD-L1）、程序性死亡配体2 （PD-L2）和细胞毒性T淋巴细胞相关蛋白4 （CTLA-4）在TCGA高血管生成HCC患者中升高，但在GSE76427队列中没有升高。结论：使用HCC患者的转录组量化血管生成表明，它与侵袭性生物学有关，但也与肿瘤免疫原性和免疫反应相关，这些免疫反应与生存相抵消，但不反映在生存中。鉴于免疫检查点分子的高表达，我们不得不推测免疫治疗可能对高血管生成的HCC患者有用。

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Angiogenesis Is Associated With Aggressive Biology That Counterbalances With Tumor Immunogenicity in Hepatocellular Carcinoma.

Background: Hepatocellular carcinoma (HCC) is an arterialized tumor; thus, anti-angiogenesis targeted therapy is in clinical practice. Herein, we hypothesized that HCC with high angiogenesis is biologically aggressive with worse survival.

Methods: Angiogenesis score (AS) was derived from the Molecular Signatures Database (MSigDB) Hallmark Angiogenesis Gene Set, and median was used to divide high versus low groups. Transcriptome of HCC patients of The Cancer Genome Atlas (TCGA, n = 386) and GSE76427 (n = 115) cohorts were analyzed.

Results: High AS correlated with angiogenesis-related gene expressions. Both microvascular and lymphatic endothelial cell infiltrations were higher in high angiogenesis HCC. Surprisingly, no survival difference was seen with varying levels of angiogenesis. High angiogenesis significantly enriched tumor aggravating signaling pathways: glycolysis, Notch, Hedgehog, KRAS, epithelial mesenchymal transition, and transforming growth factor-beta (TGF-β) in Gene Set Enrichment Analysis (GSEA), but also infiltrated less CD8⁺ T cells and T-helper 1 cells, and higher M1 macrophages and conventional dendritic cells (cDCs) with elevated cytolytic activity score in both cohorts. In agreement, immune response-related gene sets: inflammatory response, tumor necrosis factor-alpha (TNF-α) signaling, allograft rejection, interferon-alpha, and interferon-gamma were all enriched to high angiogenesis HCC. Programmed cell death protein 1 (PD1), programmed death ligand 1 (PD-L1), programmed death ligand 2 (PD-L2), and cytotoxic T lymphocyte-associated protein 4 (CTLA-4) were higher in high angiogenesis HCC in TCGA, but not in GSE76427 cohort.

Conclusions: Angiogenesis quantified using transcriptome of HCC patients demonstrated that it is associated with aggressive biology but also with tumor immunogenicity and immune response that counterbalance and did not reflect in survival. Given high expression of immune checkpoint molecules, we cannot help but speculate that immunotherapy may be useful for high angiogenesis HCC patients.

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来源期刊

World Journal of Oncology ONCOLOGY-

CiteScore

6.10

自引率

15.40%

发文量

期刊介绍： World Journal of Oncology, bimonthly, publishes original contributions describing basic research and clinical investigation of cancer, on the cellular, molecular, prevention, diagnosis, therapy and prognosis aspects. The submissions can be basic research or clinical investigation oriented. This journal welcomes those submissions focused on the clinical trials of new treatment modalities for cancer, and those submissions focused on molecular or cellular research of the oncology pathogenesis. Case reports submitted for consideration of publication should explore either a novel genomic event/description or a new safety signal from an oncolytic agent. The areas of interested manuscripts are these disciplines: tumor immunology and immunotherapy; cancer molecular pharmacology and chemotherapy; drug sensitivity and resistance; cancer epidemiology; clinical trials; cancer pathology; radiobiology and radiation oncology; solid tumor oncology; hematological malignancies; surgical oncology; pediatric oncology; molecular oncology and cancer genes; gene therapy; cancer endocrinology; cancer metastasis; prevention and diagnosis of cancer; other cancer related subjects. The types of manuscripts accepted are original article, review, editorial, short communication, case report, letter to the editor, book review.